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死后人类大脑皮层突触体对γ-氨基丁酸和L-谷氨酸的摄取:多个位点、钠依赖性及组织制备的影响

Uptake of gamma-aminobutyric acid and L-glutamic acid by synaptosomes from postmortem human cerebral cortex: multiple sites, sodium dependence and effect of tissue preparation.

作者信息

Dodd P R, Watson W E, Morrison M M, Johnston G A, Bird E D, Cowburn R F, Hardy J A

机构信息

Department of Pharmacology, University of Sydney, N.S.W., Australia.

出版信息

Brain Res. 1989 Jun 26;490(2):320-31. doi: 10.1016/0006-8993(89)90249-7.

Abstract

The uptake of gamma-aminobutyric acid (GABA) and L-glutamic acid by synaptosomes prepared from frozen postmortem human brain was shown to be effected via distinct high and low affinity sites. At approximately 17 h postmortem delay, the kinetic parameters for GABA uptake were: high affinity site, Km 7.1 +/- 2.5 microM, Vmax 18.7 +/- 4.8 nmol.min-1 per 100 mg protein; low affinity site, Km 2 +/- 1 mM, Vmax 425 +/- 250 nmol.min-1 per 100 mg protein (means +/- S.E.M., n = 13). Kinetic parameters for L-glutamate uptake were: high affinity site, Km 7.5 +/- 1.0 microM, Vmax 85 +/- 8 nmol.min-1 per 100 mg protein; low affinity site, Km 1.8 +/- 1.2 mM. Vmax 780 +/- 175 nmol.min-1 per 100 mg protein (n = 11). A detailed kinetic analysis of high affinity GABA uptake was performed over a range of sodium ion concentrations. The results were consistent with a coupling ratio of one Na+ ion to one GABA molecule; a similar result was found with rat brain synaptosomes. However, rat and human synaptosomes differed in the degree to which the substrate affinity of the high affinity GABA uptake site varied with decreasing Na+ ion concentration. High affinity GABA uptake was markedly affected by the method used to freeze and divide the tissue, but did not vary greatly in different cortical regions. There was some decline of high affinity GABA uptake activity with postmortem delay, apparently due to a loss of sites rather than a change in site affinity.

摘要

研究表明,从冷冻的人死后大脑制备的突触体对γ-氨基丁酸(GABA)和L-谷氨酸的摄取是通过不同的高亲和力和低亲和力位点进行的。在死后延迟约17小时时,GABA摄取的动力学参数为:高亲和力位点,Km 7.1±2.5微摩尔,Vmax 18.7±4.8纳摩尔·分钟-1每100毫克蛋白质;低亲和力位点,Km 2±1毫摩尔,Vmax 425±250纳摩尔·分钟-1每100毫克蛋白质(平均值±标准误,n = 13)。L-谷氨酸摄取的动力学参数为:高亲和力位点,Km 7.5±1.0微摩尔,Vmax 85±8纳摩尔·分钟-1每100毫克蛋白质;低亲和力位点,Km 1.8±1.2毫摩尔,Vmax 780±175纳摩尔·分钟-1每100毫克蛋白质(n = 11)。在一系列钠离子浓度范围内对高亲和力GABA摄取进行了详细的动力学分析。结果与一个钠离子与一个GABA分子的偶联比一致;在大鼠脑突触体中也发现了类似结果。然而,大鼠和人类突触体在高亲和力GABA摄取位点的底物亲和力随钠离子浓度降低而变化的程度上有所不同。高亲和力GABA摄取受到冷冻和分割组织所用方法的显著影响,但在不同皮质区域变化不大。随着死后延迟,高亲和力GABA摄取活性有所下降,显然是由于位点的丧失而非位点亲和力的改变。

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